Peer-reviewed veterinary case report
Genetic causes of primary hyperparathyroidism in Keeshonden dogs
By Goldstein, Richard E et al.·Published in Journal of veterinary internal medicine·2007·Department of Clinical Sciences, United States·View original on PubMed →
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Original publication title: Inheritance, mode of inheritance, and candidate genes for primary hyperparathyroidism in Keeshonden.
- Species:
- dog
Plain-English summary
A group of Keeshonden was studied for primary hyperparathyroidism (PHPT), a condition where the parathyroid glands produce too much hormone, leading to health issues. Researchers found that PHPT in Keeshonden is likely inherited in an autosomal dominant manner, meaning only one copy of the mutated gene is needed for the disease to occur. However, they did not find specific mutations in the genes they tested that would explain the condition. Identifying the exact genetic cause could help develop tests to reduce the occurrence of PHPT in this breed.
People also search for: Keeshond hyperparathyroidism symptoms · inherited diseases in Keeshonds · Keeshond genetic testing for health issues
Abstract
BACKGROUND: Primary hyperparathyroidism (PHPT) is caused by inappropriate secretion of parathyroid hormone (PTH) by autonomously functioning neoplastic or hyperplastic parathyroid "chief" cells. Keeshonden are thought to be over-represented in studies on canine PHPT, but no proof of heritability or mode of inheritance has been published. The canine disease clinically resembles human familial isolated hyperparathyroidism (FIHP). HYPOTHESIS: Primary hyperparathyroidism in Keeshonden is genetically transmitted and is caused by a mutation in 1 of 4 genes implicated in human FIHP: MEN1, CASR, HRPT2, or RET. ANIMALS: Pedigrees consisting of 1647 Keeshonden were created including 219 Keeshonden with known PHPT phenotypes (69 positive). DNA samples were obtained from 176 of the 219 Keeshonden (34 positive). METHODS: Heritability and mode of inheritance were determined by segregation analysis. Canine homologs to the human genes were identified. Exons and surrounding intron regions were sequenced and scanned for sense-altering polymorphisms or polymorphisms that segregated with the disease. Messenger RNA from a parathyroid tumor of an affected Keeshond was analyzed for polymorphisms and splice alterations. RESULTS: PHPT follows an autosomal dominant mode of inheritance in Keeshonden with possible age-dependent penetrance. No polymorphisms identified in the genes analyzed were associated with a change in predicted protein or in hypothesized splice sites. CONCLUSIONS AND CLINICAL IMPORTANCE: PHPT is an autosomal dominant, genetically transmitted disease in Keeshonden. Once the mutation locus is identified, genetic testing should quickly decrease the incidence of PHPT in this breed. It is unlikely that mutations in MEN1, CASR, HRPT2, or RET cause PHPT in Keeshonden.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/17338170/